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小鼠个体发育过程中CD4+CD8-髓质胸腺细胞的发育途径及其在Aire基因敲除小鼠中的缺陷。

Developmental pathway of CD4+CD8- medullary thymocytes during mouse ontogeny and its defect in Aire-/- mice.

作者信息

Li Juan, Li Yan, Yao Jin-Yan, Jin Rong, Zhu Ming-Zhao, Qian Xiao-Ping, Zhang Jun, Fu Yang-Xin, Wu Li, Zhang Yu, Chen Wei-Feng

机构信息

Department of Immunology, Peking University Health Science Center, 38 Xue Yuan Road, Beijing 100083, China.

出版信息

Proc Natl Acad Sci U S A. 2007 Nov 13;104(46):18175-80. doi: 10.1073/pnas.0708884104. Epub 2007 Nov 5.

Abstract

The newly generated single-positive (SP) thymocytes undergo further maturation in the thymic medulla before their emigration to the periphery. The present study was undertaken to validate a developmental program we proposed for CD4SP medullary thymocytes and to explore the mechanisms regulating this process. During mouse ontogeny, the emergence of different subsets of CD4SP thymocytes followed a strict temporal order from SP1 to SP4. Parallel to the transition in surface phenotype, a steady increase in function was observed. As further evidence, purified SP1 cells were able to sequentially give rise to SP2, SP3, and SP4 cells in intrathymic adoptive transfer and in culture. Notably, the development of CD4SP cells in the medulla seemed to be critically dependent on a functionally intact medullary epithelial cell compartment because Relb and Aire deficiency were found to cause severe blockage at the transition from SP3 to SP4. Taken together, this work establishes an ontogenetically and functionally relevant maturation program for CD4SP thymocytes. Precise dissection of this program should facilitate further inquiry into the molecular mechanisms governing normal thymocyte development and its disturbance in pathological conditions.

摘要

新产生的单阳性(SP)胸腺细胞在迁移至外周之前,会在胸腺髓质中经历进一步成熟。本研究旨在验证我们提出的CD4SP髓质胸腺细胞发育程序,并探索调节这一过程的机制。在小鼠个体发育过程中,不同亚群的CD4SP胸腺细胞按从SP1到SP4的严格时间顺序出现。与表面表型的转变平行,观察到功能稳步增强。作为进一步证据,纯化的SP1细胞在胸腺内过继转移和培养中能够依次产生SP2、SP3和SP4细胞。值得注意的是,髓质中CD4SP细胞的发育似乎严重依赖于功能完整的髓质上皮细胞区室,因为发现Relb和Aire缺陷会导致在从SP3到SP4的转变过程中出现严重阻滞。综上所述,这项工作确立了与CD4SP胸腺细胞个体发育和功能相关的成熟程序。对该程序的精确剖析应有助于进一步探究调控正常胸腺细胞发育的分子机制及其在病理条件下的紊乱情况。

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